J. Chem. Eng. Data 2004, 49, 483-485
483
Viscosities of Aqueous Solutions of Human Serum Albumin in the Presence of Two Anionic Penicillins at pH 7.4 Silvia Barbosa,* Pablo Taboada, and Vı´ctor Mosquera Grupo de Fı´sica de Coloides y Polı´meros, Departamento de Fı´sica da Materia Condensada, Facultade de Fı´sica, Universidade de Santiago de Compostela, 15782, Santiago de Compostela, Spain
Relative viscosity values for cloxacillin and dicloxacillin penicillins in an aqueous solution of pH 7.4 in the presence of human serum albumin at concentrations of 4 g L-1 and 20 g L-1 have been derived from measurements made with a microviscometer based on the “rolling ball” principle. The viscosities have been measured in the range of the temperatures (20 to 50) °C.
1. Introduction Interactions between surfactant molecules and natural polymers have been extensively reviewed.1-3 These studies have shown that complexes can be formed between proteins and surfactants in the bulk phase. Two types of protein/ surfactant interactions have been proposed: (a) specific binding via electrostatic attraction and (b) cooperative association of the surfactant to the protein via hydrophobic affinity. These interactions can give rise to important changes to the physicochemical properties of biopolymer systems and play an important role in biological and pharmacological applications. Human serum albumin (HSA) is used as a model protein for studying the interaction between proteins and different surface substrates.4,5 HSA is a globular protein that consists of 585 amino acids in a single polypeptide chain with a molar mass of 66 411 g mol-1, and it constitutes approximately half of the total blood protein, acting as carrier for fatty acids and several amphiphiles from bloodstream to tissues and hence is an appropriate choice of protein for studying the interaction with amphiphilic drugs.6-7 In this work, we report determinations of viscosities for HSA-penicillin complexes with the HSA concentration, (4 and 20) g L-1, and at the temperatures of (20, 30, 40, and 50) °C and pH 7.4. The penicillins chosen were cloxacillin and dicloxacillin, two structurally related anionic amphiphilic penicillins, which differ only in an additional chlorine atom on the phenyl ring of dicloxacillin (see Figure 1). The globular protein HSA is negatively charged at pH 7.4, and therefore only hydrophobic interactions are established between protein and the penicillins. The measurements were done above the isoelectric point of the protein (4.9) because the change in the pH alters the charge distributions of the protein molecule and hence the stability and tendency for surface adsorption.8 2. Experimental Section Materials. HSA (70024-90-7), sodium cloxacillin monohydrate (5- methyl-3-(o-chlorophenyl)-4-isoxazolyl) and sodium dicloxacillin monohydrate (3-(2,6-dichlorophenyl)5-methyl-R-isoxazolyl) with at least 98.5% purity were obtained from Sigma Chemical Company. The molecular weights of cloxacillin and dicloxacillin are 475.9 g mol-1 * To whom correspondence may be addressed. E-mail:
[email protected].
Figure 1. Molecular structure of the penicillins.
and 510.3 g mol-1, respectively. Experiments were carried out using phosphate buffered saline tablets for pH 7.4 with ionic strength of 0.188 M. The solutions were weighted on a Scaltec balance with a precision of (0.00002 g. Water was double distilled and deionized before use. Adsorption of Cloxacillin and Dicloxacillin onto HSA. Aliquots of 2 mL of 8 g L-1 (for 4 g L-1 of HSA) and 40 g L-1 (for 20 g L-1 of HSA) of HSA were added to equal volumes of aqueous solutions of penicillin of known concentration to yield final solutions that the concentrations of HSA were 4 g L-1 and 20 g L-1, respectively. The solutions were maintained at 20 °C for the necessary time until equilibrium was achieved. Viscosity. Measurements were made with an Anton Paar Automated Microviscometer (AMVn). The AMVn is based on the “rolling-ball” principle. The samples of buffer or buffer-HSA-penicillin solutions were introduced into a glass capillary with a diameter of 1.6 mm (recommended viscosity measuring range 0.3 to 10 mPa s) in which the steel ball rolls. The viscous properties of the test fluid can be determined by measuring the rolling time of the steel ball. The measurements were made in the range of temperatures from 20 °C to 50 °C. The temperature was maintained by the Peltier effect with a resolution of (0.01 °C. The precision in the measurements was (0.00004 mol kg-1 for the concentration and for the rolling time of the ball through the solution, t, of (0.002 s. For the relative viscosity, ηrel, the uncertainty is 0.10%. The rolling times of the steel ball in the buffer were (22.746 ( 0.002) s at 20 °C, (18.170 ( 0.002) s at 30 °C, (14.977 ( 0.003) s at 40 °C, and (12.681 ( 0.005) s at 50 °C in the presence of HSA at a concentration of 4 g L-1 at pH 7.4 and (24.272 ( 0.001) s at 20 °C, (19.385 ( 0.003) s at 30 °C, (15.950 ( 0.002) s at 40 °C, and (13.466 ( 0.003)
10.1021/je034143n CCC: $27.50 © 2004 American Chemical Society Published on Web 04/23/2004
484
Journal of Chemical and Engineering Data, Vol. 49, No. 3, 2004
Table 1. Concentration, c, Rolling Time of the Ball through the Solution, τ, and Relative Viscosity, ηrel, for Cloxacillin in the Presence of HSA at a Concentration of 4 and 2 g L-1 at pH 7.4 and at Different Temperatures t ) 20 °C c/(mol‚kg-1)
τ/s
t ) 30 °C ηrel
τ/s
t ) 40 °C ηrel
τ/s
0.000 48 0.001 06 0.002 08 0.005 13 0.010 12 0.019 87 0.039 91 0.099 88
22.765 22.807 22.834 22.926 23.061 23.412 24.153 26.714
1.000 83 1.002 68 1.003 87 1.007 91 1.013 85 1.029 28 1.061 86 1.174 45
Cloxacillin + 4 g L-1 HSA 18.192 1.001 21 14.988 18.227 1.003 14 15.004 18.233 1.003 47 15.020 18.306 1.007 48 15.077 18.413 1.013 37 15.161 18.684 1.028 29 15.362 19.220 1.057 79 15.778 21.139 1.163 40 17.271
0.000 52 0.002 33 0.009 73 0.024 06 0.039 36 0.098 95 0.196 96 0.297 95 0.330 14
24.377 24.396 24.712 25.213 26.344 29.721 37.041 24.377 57.015
1.004 33 1.005 11 1.018 13 1.038 77 1.085 37 1.224 50 1.526 08 1.004 33 2.349 00
Cloxacillin + 20 g L-1 HSA 19.431 1.002 37 15.991 19.483 1.005 05 16.016 19.730 1.017 80 16.235 20.106 1.037 19 16.521 20.919 1.079 13 17.137 23.368 1.205 47 19.042 29.351 1.514 11 24.025 19.431 1.002 37 15.991 44.372 2.288 99 35.485
t ) 50 °C ηrel
τ/s
ηrel
1.000 73 1.001 80 1.002 87 1.006 68 1.012 28 1.025 71 1.053 48 1.153 17
12.685 12.693 12.704 12.750 12.819 12.971 13.305 14.496
1.000 31 1.000 95 1.001 81 1.005 44 1.010 88 1.022 88 1.049 27 1.143 12
1.002 57 1.004 14 1.017 87 1.035 80 1.074 42 1.193 85 1.506 27 1.002 57 2.224 76
13.497 13.508 13.696 13.912 14.410 16.049 20.130 13.497 29.151
1.002 30 1.003 12 1.017 08 1.033 12 1.070 10 1.191 82 1.494 88 1.002 30 2.164 78
Table 2. Concentration, c, Rolling Time of the Ball through the Solution, τ, and Relative Viscosity, ηrel, for Dicloxacillin in the Presence of HSA at a Concentration of 4 and 20 g L-1 at pH 7.4 and at Different Temperatures t ) 20 °C c/(mol‚kg-1)
τ/s
t ) 30 °C ηrel
τ/s
t ) 40 °C ηrel
τ/s
0.000 53 0.000 98 0.002 06 0.005 12 0.010 10 0.019 88 0.038 51 0.099 88
22.748 22.758 22.765 22.874 23.038 23.374 24.204 27.395
1.000 09 1.000 53 1.000 83 1.005 63 1.012 84 1.027 61 1.064 10 1.204 39
Dicloxacillin + 4 g L-1 HSA 18.175 1.000 27 14.979 18.186 1.000 88 14.981 18.194 1.001 32 14.984 18.256 1.004 73 15.046 18.389 1.012 05 15.138 18.644 1.026 09 15.333 19.257 1.059 82 15.791 21.714 1.195 05 17.751
0.000 78 0.001 35 0.002 61 0.010 20 0.025 10 0.049 48 0.098 73
24.305 24.299 24.398 24.760 25.383 27.344 31.957
1.001 36 1.001 11 1.005 19 1.020 11 1.045 77 1.126 57 1.316 62
Dicloxacillin + 20 g L-1 HSA 19.395 1.000 52 15.958 19.399 1.000 72 15.969 19.458 1.003 77 16.006 19.745 1.018 57 16.241 20.200 1.042 04 16.593 21.657 1.117 20 17.720 25.306 1.305 44 20.705
t ) 50 °C ηrel
τ/s
ηrel
1.000 13 1.000 27 1.000 47 1.004 60 1.010 75 1.023 77 1.054 35 1.185 21
12.683 12.686 12.688 12.723 12.792 12.944 13.313 14.869
1.000 16 1.000 39 1.000 55 1.003 31 1.008 75 1.020 74 1.049 84 1.172 54
1.000 50 1.001 19 1.003 51 1.018 24 1.040 31 1.110 97 1.298 11
13.476 13.485 13.510 13.717 13.978 14.934 17.352
1.000 74 1.001 41 1.003 27 1.018 64 1.038 02 1.109 01 1.288 58
s at 50 °C in the presence of HSA at a concentration of 20 g L-1 at pH 7.4. 3. Results and Discussion Experimental results are given in Table 1 and Table 2 for cloxacillin and dicloxacillin at pH 7.4 and at different HSA concentrations, respectively. The relative viscosity was calculated using the equation
ηrel )
τ τ0
(1)
where τ/s is the rolling time of the ball through the solution and τ0/s is the rolling time of the ball through the buffer with the protein. In Figures 2 and 3, the increase of the relative viscosity with the concentration of cloxacillin and dicloxacillin can be observed, respectively, together with the decrease of this magnitude when the temperature increases for both HSA concentrations. Two characteristic regions are identified in both figures: (a) The first region is a plateau where viscosity remains almost constant up to concentrations close to 0.01 mol kg-1. In this region, the viscosity is almost unaffected by the presence of penicillin. (b) The second region is where the viscosity steeply rises as a consequence
Figure 2. Specific viscosity, ηrel, vs concentration, c, of cloxacillin at pH 7.4 in the presence of HSA at a concentration of (a) 4 g L-1 and (b) 20 g L-1 at different temperatures. 9, 20 °C; b, 30 °C; 2, 40 °C; 1, 50 °C.
of an increase in number and transformation in the shape of the protein molecules as has been demonstrated by dynamic light-scattering measurements.9 It has been proposed by isothermal titration calorimetry that the binding process of penicillins onto HSA can be described as a two
Journal of Chemical and Engineering Data, Vol. 49, No. 3, 2004 485 Table 3. Coefficients A1, A2, and A3 of Equation 2 for Dicloxacillin and Cloxacillin in the Presence of HSA at Concentrations 4 and 20 g L-1 at pH 7.4 and at Different Temperatures 4 g L-1 HSA A1
A2
20 g L-1 HSA A3
t ) 20 °C t ) 30 °C t ) 40 °C t ) 50 °C
0.767 ( 0.030 0.805 ( 0.026 0.847 ( 0.013 0.871 ( 0.017
0.231 ( 0.030 0.193 ( 0.022 0.152 ( 0.013 0.127 ( 0.016
Dicloxacillin 0.157 ( 0.015 0.142 ( 0.012 0.124 ( 0.007 0.115 ( 0.010
t ) 20 °C t ) 30 °C t ) 40 °C t ) 50 °C
0.668 ( 0.035 0.692 ( 0.032 0.724 ( 0.014 0.760 ( 0.001
0.332 ( 0.035 0.309 ( 0.032 0.276 ( 0.014 0.239 ( 0.010
Cloxacillin 0.237 ( 0.021 0.236 ( 0.020 0.226 ( 0.009 0.212 ( 0.007
A1
A2
A3
0.791 ( 0.048 0.830 ( 0.033 0.855 ( 0.024 0.855 ( 0.031
0.207 ( 0.046 0.168 ( 0.031 0.143 ( 0023 0.143 ( 0.030
0.106 ( 0.015 0.095 ( 0.011 0.088 ( 0.008 0.083 ( 0.011
0.693 ( 0.032 0.689 ( 0.017 0.665 ( 0.013 0.634 ( 0.015
0.312 ( 0.029 0.314 ( 0.015 0.336 ( 0.012 0.364 ( 0.014
0.198 ( 0.009 0.203 ( 0.005 0.215 ( 0.004 0.230 ( 0.047
for binding and, thus, delays the configuration changes of the protein. The differences between the relative viscosities of the protein at the concentration of 20 g L-1 and in the presence of some of the penicillins in the temperature range of the present study are minimum. Literature Cited
Figure 3. Specific viscosity, ηrel, vs concentration, c, for dicloxacillin at pH 7.4 in the presence of HSA at a concentration of (a) 4 g L-1 and (b) 20 g L-1 at different temperatures. 9, 20 °C; b, 30 °C; 2, 40 °C; 1, 50 °C.
binding site model, in which the first site would bind just one penicillin molecule and the second site the rest of the adsorbed penicillin molecules (about 15-25 penicillin molecules depending on the compound).10-11 The variation of the relative viscosity with the penicillin concentration, c, can be described by the exponential equation
ηrel ) A1 + A2 ec/A3
(2)
with values of the coefficients A1, A2, and A3 given in Table 3. The effect of protein concentration can be observed in the Figures 2 and 3. At 20 g L-1 of protein, the plateau extends to a higher penicillin concentration as a consequence of the existence of more protein molecules available
(1) Tanford, C. The Hydrophobic Effect: Formation of Micelles and Biological Membranes; Willey Interscience: New York, 1980. (2) Ananthapadmanabham, K. P. Interactions of Surfactants with Polymers and Proteins; Goddard, E. D., Ananthapadmanabhan D. P., Eds.; CRC Press, Inc.: London, 1993. (3) Kwak, J. C. T. Polymer-Surfactant Systems; Surfactant Science Series; Kwak, J. C. T., Ed.; Marcel Dekker: New York, 1998; Vol. 77. (4) Peters, T. J. All About Albumin Biochemistry, Genetics, and Medical Applications; Academic Press: San Diego, CA, 1996. (5) Taboada, P.; Mosquera, V.; Ruso, J. M.; Sarmiento, F.; Jones, M. N. Interaction between Penicillins and Human Serum Albumin: A Thermodynamic Study of Micellar-Like Clusters on a Protein. Langmuir 2000, 16, 934-938. (6) Taboada, P.; Mosquera, V.; Ruso, J. M.; Sarmiento, F.; Jones, M. N. Interaction between Penicillins and Human Serum Albumin: A ξ-Potential Study. Langmuir 2000, 16, 6795-6800. (7) Barbosa, S.; Leis, D.; Taboada, P.; Atwood, D.; Mosquera, V. A Study of the Adsorption of the Amphiphilic Penicillins Cloxacillin and Dicloxacill onto Human Serum Albumin using Surface Tension Isotherms. Mol. Phys. 2002, 21, 3367-3374. (8) Lu, J. R.; Su, T. J. and Penfold, J. Adsorption of Serum Albumins at the Air/Water Interface. Langmuir 1999, 15, 6975-6983. (9) Ruso, J. M.; Attwood, D.; Garcı´a, M.; Taboada, P.; Varela, L. M.; Mosquera, V. A Study of the Interaction of the Amphiphilic Penicillins Cloxacillin and Dicloxacillin whith Human Serum Albumin in Aqueous Solution. Langmuir 2001, 17, 5189-5195. (10) Landau, M. A.; Markovich, M. N.; Piruzyan, L. A. Studies of the Thermodinamics and Nature of Interaction between Serum Albumin and Penicillins. Biochim. Biophys. Acta 1977, 493, 1-9. (11) Barbosa, S.; Taboada, P.; Mosquera, V. Protein-Ligand Interactions: Volumetric and Compressibility Characterization of the Binding of Two Anionic Penicillins to Human Serum Albumin. Langmuir 2003, 19, 1446-1448. Received for review July 23, 2003. Accepted March 22, 2004.
JE034143N